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Evidence to suggest that cathepsin K degrades articular cartilage in naturally occurring equine osteoarthritis.

机译:有证据表明组织蛋白酶K可在自然发生的马骨关节炎中降解关节软骨。

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OBJECTIVE: The mechanisms leading to degeneration of articular cartilage in osteoarthritis (OA) are complex and not yet fully understood. Cathepsin K (CK) is a cysteine protease which can also cleave the triple helix of type II collagen. This exposes a neoepitope that can now be identified by specific antibodies. The aim of this study was to obtain evidence suggesting a role for CK in naturally occurring equine OA in both lesional and peri-lesional regions. METHODS: Articular cartilages (n=12 horses; 5 healthy, 7 OA) were harvested from animals postmortem. A gross macroscopic examination, histologic (Safranin O-Fast Green and Picrosirius red staining) and immunohistochemical evaluation were performed. Samples were divided into normal appearing cartilage, peri-lesional and lesional cartilage. Cartilage degradation in the samples was graded histologically and immunohistochemically. CK and possible CK cleavage were detected immunohistochemically with specific anti-protein and anti-neoepitope antibodies, respectively. A comparison of CK neoepitope (C2K) production with the collagenase-generated neoepitope produced by matrix metalloproteinases (MMP)-1, 8 and 13 (C2C) was also assessed immunohistochemically. RESULTS: CK and CK cleavage were significantly more abundant in OA cartilage (both peri-lesional and lesional) when compared to remote cartilage within the sample joint or cartilage from healthy joints. The immunohistochemical pattern observed for CK degradation (C2K) was similar to that of collagenase degradation (C2C). Macroscopic cartilage changes and histologic findings were significantly correlated with immunohistochemistry results. CONCLUSION: The data generated suggests that CK may be involved in cartilage collagen degradation in naturally occurring osteoarthritis.
机译:目的:骨关节炎(OA)中导致关节软骨退变的机制很复杂,尚未完全了解。组织蛋白酶K(CK)是一种半胱氨酸蛋白酶,还可以切割II型胶原蛋白的三螺旋。这暴露了新表位,该表位现在可以通过特异性抗体鉴定。这项研究的目的是获得证据表明在病变和病变周围区域CK在自然存在的马OA中的作用。方法:从死后的动物中收集关节软骨(n = 12匹马; 5头健康,7 OA)。进行了肉眼宏观检查,组织学检查(番红O型快速绿和皮克西里乌斯红染色)和免疫组化评估。将样品分为正常出现的软骨,病灶周围和病灶软骨。对样品中的软骨降解进行组织学和免疫组织化学分级。用特异性抗蛋白和抗新表位抗体分别免疫组织化学检测CK和可能的CK裂解。免疫组织化学还评估了CK新表位(C2K)产生与由基质金属蛋白酶(MMP)-1、8和13(C2C)产生的胶原酶产生的新表位的比较。结果:与样本关节内的远端软骨或健康关节的软骨相比,OA软骨(病灶周围和病灶)的CK和CK裂解明显丰富。观察到的CK降解(C2K)的免疫组织化学模式与胶原酶降解(C2C)相似。宏观软骨变化和组织学结果与免疫组织化学结果显着相关。结论:产生的数据表明CK可能参与天然骨关节炎中软骨胶原蛋白的降解。

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